However, common sense
alone raises questions about the dangers of foreign DNA - otherwise
known as recombinant DNA. The American Biologic Safety Association
(ABSA) has classified recombinant DNA a biohazard and has outlined
specific directives over the handling of such contaminants.1

“…The presence of dormant and relict viral sequences in the human
and other animal genomes has been known for at least 20 years. These
include human retroviral sequences that have been identified in live
viral vaccines grown in human cells.
2

“Victoria
and colleagues have identified the contamination of live viral
vaccines for use in healthy children, with viral nucleic acids; the
findings have since been confirmed by the vaccine
manufacturers and the data reported to the FDA.
Contaminating nucleic acids include retroviral sequences from the
producer chicken and primate cells.

Since this
report, a second rotavirus vaccine (RotaTeq) has been shown
to contain nucleic acids from both PCV1 and PCV2, a pathogen in pigs
that is associated with wasting and immunodeficiency. The
circumstances in which PCV2 induces disease are discussed below.“3

The Center for the
Biology of Chronic
Disease (CBCD),* publisher of Dr. Hanan Polansky’s the Purple
book Microcompetition with Foreign DNA and the Origin of Chronic
Disease explains how foreign DNA fragments can cause many major
diseases without damaging (mutating) the human DNA.

The book has been read by more than 5,000 scientists
around the world, and has been reviewed in more than 20 leading
scientific journals.The theory explains the underlying
cause of many major diseases and shows how dormant viruses
actually can cause disease while still latent.

Dr. Polanskydiscovered that foreign DNA fragments called N-boxes can cause
disease. When these foreign DNA fragments enter the body (naturally,
or artificially, like through an injection of a vaccine or other
treatments), they end up in the cell’s nucleus, where they attract
scarce genetic resources.

The “microcompetition” between the foreign
N-boxes and the human N-boxes cause the human genes to malfunction,
which, in turn, can lead to
disease.

In fact, when approached
about the HPV rDNA contamination found in Gardasil® - Dr. Polansky
agreed that the contaminant should not be there.

According to Polansky - the potentially harmful contaminant is part of the faulty
biologic medicine manufacturing process that is unable to filter out
all foreign DNA plasmids and therefore the particles were suspected
to be present in all biologic medicines on the market.

In April of this year,
the CBCD published a press release4 encouraging the CDC
to study Polansky’s Microcompetition Theory since foreign
DNA has also been found in Merck & Co.’s MMR II vaccine.5

The vaccine package insert (available for download at the
FDA’s web site) shows that fetal cell line Wistar RA 27/3, fetal
cell line WI-38, and genetically engineered human albumin are all
used in the vaccine.

The CBCD believes that a
better understanding of the theory - lauded by many scientists and
researchers at NIH, and other esteemed universities and
organizations may lead to better policies to curb the Autism
epidemic. In a recent CDC report that epidemic has increased by 78%
since 2007.

Infants 12 months of age
or older, are inoculated with the MMR II vaccine with a second dose
usually given around age four or five right before entry to school.
According to the CBCD, this is also usually the time that the
majority of Autism diagnoses are made.

The release goes on to
state:

The CBCD believes that
the current purification processes cannot completely filter all
foreign DNA plasmids used in the process of manufacturing the MMR II
vaccine. Therefore, some foreign DNA fragments end up being injected
into infants.

“The MMR II
vaccine is contaminated with human DNA from the cell line in which
the rubella virus
is grown. This human DNA could be the cause of the spikes in
incidence.

An additional increased spike in incidence of autism
occurred in 1995 when the chicken pox vaccine was grown in human
fetal tissue,” wrote Dr. Helen Ratajczak, Ph.D. in support of this
belief. She published two papers regarding this subject in the Journal of Immunotoxicology. (Merck and Co. Inc., 2001; Breuer,
2003)

However, it appears that
the CDC and FDA are aware of the problem with vaccines.

In June of
2001, a paper was published in Emerging Infectious Diseases
entitled: “Adventitious Agents and Vaccines” stating that:

“Many novel
vaccines are produced in animal cell substrates, and emerging
infectious diseases may theoretically be transmitted from animals to
humans through these vaccines.

Dormant HPV
Infections the Silent Culprit

Although the FDA
asserts that the foreign DNA fragments
found in Gardasil®poses no
risk, the CBCD disagrees.

Their research has led them to believe
that HPV has the ability to establish a chronic, dormant (latent)
infection and it those chronic infections that can potentially lead
to cancer.

A recent study entitled
“Prevalence of Oral HPV Infection in the United States, 2009 - 2010”
that was published in the Journal of the American Medical
Association (JAMA) reported that the HPV virus was found in the
mouths of 7% of study participants. 5,600 people participated in the
study.

Oral HPV was found in men more than in women.

The authors of the study
wrote,

‘The prevalence of oral HPV infection among men and women
aged 14 to 69 years in the United States is approximately 7%…
Infection with HPV-16, (a specific type of HPV most associated with
cancer) was detected in 1% of men and women, corresponding to an
estimated 2.13 million infected individuals in the United States.’

In essence,
according to the study, 2.13 million people who don’t have symptoms
now, and don’t even know they are infected, could develop cancer due
to their HPV infection. 7

Now add in the
rDNA factor and one has to wonder at the mechanisms of action that
are actually going on in the body.

Dormant DNA - potentially
becoming stimulated by the vaccine designed to prevent the chronic
infection leading to cervical and other HPV-related cancers - with a
mix of rDNA bound to aluminum now circulating in the blood and
targeting the weakened areas of the body.

HPV rDNA
Particles found in Postmortem Inquest of New Zealand Girl

In August, Dr Sin
Hang Lee, a pathologist on the medical staff at Connecticut’s
Milford Hospital testified about the discovery of HPV DNA fragments
in post-mortem samples of her blood and spleen 6 months after
Gardasil®® vaccination at the postmortem inquest of
Jasmine Renata, a New Zealand teenager who died in her sleep.8

Dr. Lee’s testimony
stated:

“The finding of these
foreign DNA fragments in the post-mortem samples six months after
vaccination indicates that some of the residual DNA fragments from
the viral gene or plasmid injected with Gardasil® have
been protected from degradation in the form of DNA-aluminum
complexes in the macrophages; or via integration into the human
genome.

Undegraded viral and
plasmid DNA fragments are known to activate macrophages, causing
them to release tumor necrosis factor, a myocardial depressant which
can induce lethal shock in animals and humans.”

Although Dr. Lee’s
discovery cannot directly tie the rDNA to the girl’s death, the
probable mechanism of action does exist since all other ‘cause of
death’ scenarios have been ruled out.

According to Dr. Lee,
Gardasil® contains a genetically engineered recombinant HPV DNA
inserted into yeast cells. rDNA behaves differently than natural HPV
DNA which does not stay in the blood stream for a long period of
time.

Once a segment of
recombinant DNA is inserted into a human cell, the consequences are
hard to predict.

It may be in the cell temporarily or stay there
forever, with or without causing a mutation. Now the host cell
contains human DNA as well as genetically engineered viral DNA.
9

War of the DNA

The most frightening
aspect of all is that government health agencies do not have the
testing nor do they have understanding as to what happens when a
recombinant DNA particle infects a cell with ‘normal’ DNA.

What are
the mechanisms of action that determine who wins the DNA wars? What
if the normal ‘DNA’ loses? Are the skyrocketing rates of autism and
the increasing Post-Gardasil and Post-Cervarix Syndromes examples of
DNA gone bad?

Even more frightening is
that scientists do not know how to isolate or even remove the
foreign DNA particles from the body.

What lies ahead is a crap shoot
for medical consumers who are left with a,

** Note: As of
mid-August the CBCD have stopped answering their phones. In fact,
upon calling - one gets a recorded message saying ‘this phone call
may be recorded’ even before hearing the dial tone. I was told that
Dr. Polansky was going to approve my article. However, all email
communications have now ceased.

CBCD
Suggests CDC Study Microcompetition Theory

The Center
for the Biology of Chronic Disease (CBCD) believes that
the cause of the epidemic is the foreign DNA

in the MMR
II vaccine.

The CDC’s latest report
on Autism says,

“More children than
ever before are being diagnosed with autism spectrum disorders (ASDs).
Like the many families living with ASDs, CDC considers ASDs an
important public health concern.” [1]

Autism rates have gone
up by 25% in just two years. In fact, the latest CDC report marks a
78% increase since its first report on Autism in 2007. Experts call
it an epidemic. The Center for the Biology of Chronic Disease (CBCD)
believes that the cause of the epidemic is the foreign DNA in the
MMR II vaccine.

The CDC must be aware of
the existence of foreign DNA in the MMR II vaccine. However, the CDC
may be unaware of the relationship between foreign DNA and Autism as
explained by the Microcompetition theory.

The CDC is aware of the
public demand to find the cause of the epidemic.

According to the
CDC,

“The CDC knows that people want answers to what is causing the
increase in the number of children identified with ASDs and so do
we.”

The CBCD urges CDC
officials to become familiar with the Microcompetition theory as
described in Dr. Hanan Polansky’s “Purple Book,” which has been
available as a free public access download from the CBCD website
since 2003.

“At first, I wish to
congratulate Dr. Hanan Polansky for his scientific bravery to take
such a unique, novel approach to further stimulate our understanding
of the origin and establishment of chronic diseases. The philosophy
underscored is an excellent one…

The amazing correlation between
theoretical predictions and observed in vivo effects seem to bring
us a step closer to a deeper understanding of such complex biologic
processes,” said Dr. Sivasubramanian Baskar, PhD, a Senior Scientist
at the National Cancer Institute, NIH.

A better understanding
of the theory may lead to better policies to curb the Autism
epidemic.

As mentioned above, the
MMR II vaccine contains foreign DNA fragments. The MMR II vaccine is
given to infants 12 months of age or older, with a second dose
usually given around age four or five right before starting school.
Perhaps not so coincidentally, this is also usually the time that
the majority of Autism diagnoses are made.

Surely, the CDC knows
that information regarding DNA fragments contaminating the MMR II is
available to the public as a download from the FDA’s website.
[2]

One can download the vaccine package insert for the MMR II vaccine
written by Merck & Co., Inc. which shows that Fetal cell line Wistar
RA 27/3, Fetal cell line WI-38, and genetically engineered human
albumin are all used in the vaccine.

The CBCD believes that
the current purification processes cannot completely filter all
foreign DNA plasmids used in the process of manufacturing the MMR II
vaccine.

Therefore, some foreign DNA fragments end up being injected
into infants.

“The MMR II vaccine is
contaminated with human DNA from the cell line in which the rubella
virus is grown. This human DNA could be the cause of the spikes in
incidence. An additional increased spike in incidence of autism
occurred in 1995 when the chicken pox vaccine was grown in human
fetal tissue,” wrote Dr. Helen Ratajczak, Ph.D. in support of this
belief. She published two papers regarding this subject in the
Journal of Immunotoxicology.

(Merck and Co., Inc., 2001; Breuer,
2003).

Microcompetition between
the foreign DNA fragments injected into infants through the MMR II
vaccine and the child’s own DNA could be the biological mechanism
linking the MMR II vaccine to Autism.

With the above
information in mind, the CBCD especially encourages the CDC and NHS
to conduct research into this area and fund studies to either
confirm or deny the CBCD’s suspicions.

The CBCD also encourages
CDC, NHS, and FDA officials, as well as virologists, biologists,
geneticists, scientists, physicians and the public to obtain a copy
of Dr. Hanan Polansky’s book and read it.

The CBCD endorses Dr.
Polansky’s theory and invites family doctors, pediatricians,
scientists, the media, and the public to contact us on this issue.

For more
information on the Center for the Biology of Chronic Disease, or to
schedule an interview with Dr. Polansky, please visit http://www.cbcd.net
or call 585-250-9999.

The Center for the Biology of Chronic Disease (CBCD, http://www.cbcd.net)
is a research center recognized by the IRS as a 501(c)(3)
non-for-profit organization. The mission of the CBCD is to
advance the research on the biology of chronic diseases, and to
accelerate the discovery of treatments for these diseases.

The CBCD published
the “Purple” book entitled “Microcompetition with Foreign DNA
and the Origin of Chronic Disease” written by Dr. Hanan Polansky.
The book presents Dr. Polansky’s highly acclaimed scientific
theory on the relationship between the DNA of latent (chronic)
viruses and the onset of chronic diseases. Dr. Polansky’s book
is available as a free download from the CBCD website.